老年性黄斑变性中dren和亚rpe沉积物的高光谱自身荧光特征。

Annals of Eye Science Pub Date : 2021-03-01 Epub Date: 2021-03-15 DOI:10.21037/aes-20-12
Yuehong Tong, Thomas Ach, Christine A Curcio, R Theodore Smith
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引用次数: 5

摘要

背景:软瘤和基底线性沉积(BLinD)是两种形式的细胞外富脂物质,它们共同构成了布鲁氏膜上的溢油(BrM)。结节是局灶性的,可在临床上识别。相比之下,BLinD呈薄而弥漫性分布,即使在最高分辨率的OCT下也不可见,但在离体高光谱自体荧光(AF)成像中可以检测到。我们试图优化组织高光谱AF成像和图像分析,以识别dren和亚rpe沉积物(包括BLinD和基底层流沉积物),以用于潜在的临床应用。方法:对4例AMD供体RPE/BrM平板支架上的20个特异病灶和12个特异病灶,分别在4种激发波长(λex 436、450、480和505 nm)下进行高光谱自动对焦成像,并采用非负矩阵分解(NMF)方法对图像立方体进行分解。每个激发波长选取4个发射光谱的4阶恢复。结果:在所有含drusen的组织中均获得了对drusen和推定亚rpe矿床敏感且特异的复合发射光谱(SDr光谱),其峰值在510 ~ 520 nm处,在λ ex436、450和480 nm处振幅最大。联合源脂褐素(LF)/黑脂褐素(MLF)的RPE光谱具有相当的振幅,并且一致地再现了先前报道的所有组织的光谱S1、S2和S3:具有结节、中央凹和中央凹外位置的组织。结论:临床高光谱AF相机,在适当选择蓝色范围内的激发波长和高光谱AF检测器,应该能够检测和量化黄斑变性和亚rpe沉积,这是AMD最早已知的病变,比任何其他现有的成像方式都要早。
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Hyperspectral autofluorescence characterization of drusen and sub-RPE deposits in age-related macular degeneration.

Background: Soft drusen and basal linear deposit (BLinD) are two forms of the same extracellular lipid rich material that together make up an Oil Spill on Bruch's membrane (BrM). Drusen are focal and can be recognized clinically. In contrast BLinD is thin and diffusely distributed, and invisible clinically, even on highest resolution OCT, but has been detected on en face hyperspectral autofluorescence (AF) imaging ex vivo. We sought to optimize histologic hyperspectral AF imaging and image analysis for recognition of drusen and sub-RPE deposits (including BLinD and basal laminar deposit), for potential clinical application.

Methods: Twenty locations specifically with drusen and 12 additional locations specifically from fovea, perifovea and mid-periphery from RPE/BrM flatmounts from 4 AMD donors underwent hyperspectral AF imaging with 4 excitation wavelengths (λex 436, 450, 480 and 505 nm), and the resulting image cubes were simultaneously decomposed with our published non-negative matrix factorization (NMF). Rank 4 recovery of 4 emission spectra was chosen for each excitation wavelength.

Results: A composite emission spectrum, sensitive and specific for drusen and presumed sub-RPE deposits (the SDr spectrum) was recovered with peak at 510-520 nm in all tissues with drusen, with greatest amplitudes at excitations λex 436, 450 and 480 nm. The RPE spectra of combined sources Lipofuscin (LF)/Melanolipofuscin (MLF) were of comparable amplitude and consistently recapitulated the spectra S1, S2 and S3 previously reported from all tissues: tissues with drusen, foveal and extra-foveal locations.

Conclusions: A clinical hyperspectral AF camera, with properly chosen excitation wavelengths in the blue range and a hyperspectral AF detector, should be capable of detecting and quantifying drusen and sub-RPE deposits, the earliest known lesions of AMD, before any other currently available imaging modality.

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